Native lamin A/C proteomes and novel partners from heart and skeletal muscle in a mouse chronic inflammation model of human frailty

Elzamzami, Fatima D.; Samal, Arushi; Arun, Adith S.; Dharmaraj, Tejas; Prasad, Neeti R.; Rendon-Jonguitud, Alex; DeVine, Lauren; Walston, Jeremy D.; Cole, Robert N.; Wilson, Katherine L.

doi:10.3389/fcell.2023.1240285

Front. Cell Dev. Biol.

2023

DOI: 10.3389/fcell.2023.1240285

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Native lamin A/C proteomes and novel partners from heart and skeletal muscle in a mouse chronic inflammation model of human frailty

Fatima D. Elzamzami,

Arushi Samal,

Adith S. Arun

et al.

Abstract: Clinical frailty affects ∼10% of people over age 65 and is studied in a chronically inflamed (Interleukin-10 knockout; “IL10-KO”) mouse model. Frailty phenotypes overlap the spectrum of diseases (“laminopathies”) caused by mutations in LMNA. LMNA encodes nuclear intermediate filament proteins lamin A and lamin C (“lamin A/C”), important for tissue-specific signaling, metabolism and chromatin regulation. We hypothesized that wildtype lamin A/C associations with tissue-specific partners are perturbed by chronic … Show more

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2024

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Cited by 3 publications

References 141 publications

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FAM210A: An emerging regulator of mitochondrial homeostasis

Wang,

Yue

2024

BioEssays

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Mitochondrial homeostasis serves as a cornerstone of cellular function, orchestrating a delicate balance between energy production, redox status, and cellular signaling transduction. This equilibrium involves a myriad of interconnected processes, including mitochondrial dynamics, quality control mechanisms, and biogenesis and degradation. Perturbations in mitochondrial homeostasis have been implicated in a wide range of diseases, including neurodegenerative diseases, metabolic syndromes, and aging‐related disorders. In the past decades, the discovery of numerous mitochondrial proteins and signaling has led to a more complete understanding of the intricate mechanisms underlying mitochondrial homeostasis. Recent studies have revealed that Family with sequence similarity 210 member A (FAM210A) is a novel nuclear‐encoded mitochondrial protein involved in multiple aspects of mitochondrial homeostasis, including mitochondrial quality control, dynamics, cristae remodeling, metabolism, and proteostasis. Here, we review the function and physiological role of FAM210A in cellular and organismal health. This review discusses how FAM210A acts as a regulator on mitochondrial inner membrane to coordinate mitochondrial dynamics and metabolism.

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FAM210A: An emerging regulator of mitochondrial homeostasis

Wang,

Yue

2024

BioEssays

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Recent insights in striated muscle laminopathies

Leconte,

Bonne,

Bertrand

2024

Current Opinion in Neurology

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Purpose of review To highlight recent insights in different aspects of striated muscle laminopathies (SMLs) related to LMNA mutations. Recent findings Clinical and genetic studies allow better patient management and diagnosis, with confirmation of ventricular tachyarrhythmias (VTA) risk prediction score to help with ICD implantation and development of models to help with classification of LMNA variants of uncertain significance. From a pathophysiology perspective, characterization of lamin interactomes in different contexts revealed new lamin A/C partners. Expression or function modulation of these partners evidenced them as potential therapeutic targets. After a positive phase 2, the first phase 3 clinical trial, testing a p38 inhibitor targeting the life-threatening cardiac disease of SML, has been recently stopped, thus highlighting the need for new therapeutic approaches together with new animal and cell models. Summary Since the first LMNA mutation report in 1999, lamin A/C structure and functions have been actively explored to understand the SML pathophysiology. The latest discoveries of partners and altered pathways, highlight the importance of lamin A/C at the nuclear periphery and in the nucleoplasm. Modulation of altered pathways allowed some benefits, especially for cardiac involvement. However, additional studies are still needed to fully assess treatment efficacy and safety.

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PERM1—An Emerging Transcriptional Regulator of Mitochondrial Biogenesis: A Systematic Review

Soares Menezes,

Wu,

Renwick

et al. 2024

Genes

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Background/Objectives: This systematic review aims to explore the role of PERM1 across different organisms, tissues, and cellular functions, with a particular focus on its involvement in regulating skeletal muscle mitochondrial biogenesis. Methods: This systematic review follows The PRISMA 2020 Statement. We used the Covidence systematic review software for abstract/title screening, full-text review, and data extraction. The review included studies that examined PERM1 expression or activity in skeletal muscle, heart, and adipose tissue and/or cells, from mice, rats, and humans, and involved exercise or disease models. Risk of bias was assessed using the Cochrane Collaboration tool, and the data were extracted and synthesized qualitatively, with bioinformatic analyses performed using the MetaMEx database. Results: Twenty-one studies were included in our data extraction process, where 10 studies involved humans, 21 involved mice, four involved rats, and 11 involved cells. Conclusions: PERM1 in skeletal muscle increases with endurance exercise, affecting muscle function and oxidative metabolism, but its role in humans is not well understood. In cardiac tissue, PERM1 is vital for function and mitochondrial biogenesis purposes, but decreases with disease and pressure overload. Our review synthesizes the current understanding of PERM1’s function, raises awareness of its role in mitochondrial regulation, and identifies key areas for future research in the field.

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Native lamin A/C proteomes and novel partners from heart and skeletal muscle in a mouse chronic inflammation model of human frailty

Cited by 3 publications

References 141 publications

FAM210A: An emerging regulator of mitochondrial homeostasis

FAM210A: An emerging regulator of mitochondrial homeostasis

Recent insights in striated muscle laminopathies

PERM1—An Emerging Transcriptional Regulator of Mitochondrial Biogenesis: A Systematic Review

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